An anion-selective analogue of the channel-forming peptide alamethicin. |
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| Authors: | A V Starostin R Butan V Borisenko D A James H Wenschuh M S Sansom G A Woolley |
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| Institution: | Department of Chemistry, University of Toronto, 80 St. George Street, Toronto M5S 3H6, Canada. |
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| Abstract: | The peptide alamethicin self-assembles to form helix bundle ion channels in membranes. Previous macroscopic measurements have shown that these channels are mildly cation-selective. Models indicate that a source of cation selectivity is a zone of partial negative charge toward the C-terminal end of the peptide. We synthesized an alamethicin derivative with a lysine in this zone (replacing the glutamine at position 18 in the sequence). Microscopic (single-channel) measurements demonstrate that dimeric alamethicin-lysine18 (alm-K18) forms mildly anion-selective channels under conditions where channels formed by the parent peptide are cation-selective. Long-range electrostatic interactions can explain the inversion of ion selectivity and the conductance properties of alamethicin channels. |
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